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首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >A hairpin turn in a class II MHC-bound peptide orients residues outside the binding groove for T cell recognition.
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A hairpin turn in a class II MHC-bound peptide orients residues outside the binding groove for T cell recognition.

机译:II类MHC结合的肽中的发夹状转子将残基定向在结合槽外以进行T细胞识别。

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摘要

T cells generally recognize peptide antigens bound to MHC proteins through contacts with residues found within or immediately flanking the seven- to nine-residue sequence accommodated in the MHC peptide-binding groove. However, some T cells require peptide residues outside this region for activation, the structural basis for which is unknown. Here, we have investigated a HIV Gag-specific T cell clone that requires an unusually long peptide antigen for activation. The crystal structure of a minimally antigenic 16-mer bound to HLA-DR1 shows that the peptide C-terminal region bends sharply into a hairpin turn as it exits the binding site, orienting peptide residues outside the MHC-binding region in position to interact with a T cell receptor. Peptide truncation and substitution studies show that both the hairpin turn and the extreme C-terminal residues are required for T cell activation. These results demonstrate a previously unrecognized mode of MHC-peptide-T cell receptor interaction.
机译:T细胞通常通过与在MHC肽结合槽中容纳的7至9个残基序列中发现的残基接触或与之紧邻的残基接触,识别与MHC蛋白结合的肽抗原。然而,一些T细胞需要该区域外的肽残基来激活,其结构基础尚不清楚。在这里,我们研究了HIV Gag特异性T细胞克隆,该克隆需要异常长的肽抗原才能激活。与HLA-DR1结合的最小抗原性16-mer的晶体结构表明,肽C末端区域离开结合位点时会急剧弯曲成发夹状转弯,使MHC结合区域外的肽残基定向在与之相互作用的位置T细胞受体。肽截短和取代研究表明,发夹转向和极端的C末端残基都需要T细胞激活。这些结果证明了以前无法识别的MHC-肽-T细胞受体相互作用的模式。

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